Phenotypic mixing and hiding may contribute to memory in viral quasispecies

doi:10.1186/1471-2180-3-11

BMC Microbiology
Volume 3

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Research article

Phenotypic mixing and hiding may contribute to memory in viral quasispecies

Claus O Wilke¹ and Isabel S Novella²

¹Digital Life Laboratory, California Institute of Technology, Mail Code 136-93, Pasadena, California 91125, USA

²Department of Microbiology and Immunology, Medical College of Ohio, Toledo, Ohio 43614, USA

author email corresponding author email

BMC Microbiology 2003, 3:11doi:10.1186/1471-2180-3-11


Published:	9 June 2003

Abstract

Background

In a number of recent experiments with food-and-mouth disease virus, a deleterious mutant, RED, was found to avoid extinction and remain in the population for long periods of time. Since RED characterizes the past evolutionary history of the population, this observation was called quasispecies memory. While the quasispecies theory predicts the existence of these memory genomes, there is a disagreement between the expected and observed mutant frequency values. Therefore, the origin of quasispecies memory is not fully understood.

Results

We propose and analyze a simple model of complementation between the wild type virus and a mutant that has an impaired ability of cell entry, the likely cause of fitness differences between wild type and RED mutants. The mutant will go extinct unless it is recreated from the wild type through mutations. However, under phenotypic mixing-and-hiding as a mechanism of complementation, the time to extinction in the absence of mutations increases with increasing multiplicity of infection (m.o.i.). If the RED mutant is constantly recreated by mutations, then its frequency at equilibrium under selection-mutation balance also increases with increasing m.o.i. At high m.o.i., a large fraction of mutant genomes are encapsidated with wild-type protein, which enables them to infect cells as efficiently as the wild type virions, and thus increases their fitness to the wild-type level. Moreover, even at low m.o.i. the equilibrium frequency of the mutant is higher than predicted by the standard quasispecies model, because a fraction of mutant virions generated from wild-type parents will also be encapsidated by wild-type protein.

Conclusions

Our model predicts that phenotypic hiding will strongly influence the population dynamics of viruses, particularly at high m.o.i., and will also have important effects on the mutation-selection balance at low m.o.i. The delay in mutant extinction and increase in mutant frequencies at equilibrium may, at least in part, explain memory in quasispecies populations.